I heard about Live Blood Analysis, and I checked the web, but there so many different informations:live blood analysis review, live blood analysis training, live blood analysis pictures

From Wikipedia, the free encyclopediaJump to: navigation, searchLive Blood Analysis (LBA), sometimes called Live Blood Cell Analysis http://www.dreddyclinic.com/integrated_med/live_blood.php, is the high resolution microscopic observation of live blood cells in a dark field, a common technique in microbiology called dark field microscopy.

It is an unestablished diagnostic test used by some health care practitioners to determine a course of treatment. A drop of blood is taken from the patient's fingertip, put on a glass plate and viewed via a microscope on a video screen.

Proponents believe that the method provides information "about the state of the immune system, possible vitamin deficiencies, amount of toxicity, pH and mineral imbalance, areas of concern and weaknesses, fungus and yeast." Some even claim it can "spot cancer and other degenerative immune system diseases up to two years before they would otherwise be detectable"; or say they can diagnose "lack of oxygen in the blood, low trace minerals, lack of exercise, too much alcohol or yeast, weak kidneys, bladder or spleen". While advocates of LBA continue to insist that it is a diagnostic method "valuable for the early detection of serious health conditions," Edzard Ernst, professor of complementary medicine at the Peninsula medical school at the University of Exeter and University of Plymouth notes that "No credible scientific studies have demonstrated the reliability of LBA for detecting any of the above conditions."

Researchers at the department of physiology and pharmacology at the Sackler faculty of medicine, University of Tel Aviv have reported that "the observation of low-frequency fluctuations of the cell membrane in erythrocytes and in several nucleated cells '(white blood cell)' suggest that this phenomenon may be a general property of the living cell. A study of these fluctuations in human erythrocytes and it's ghosts have now been carried out using a novel optical method based on point dark field microscopy."

I have basic training in microscopy in US. I'm also a practicing naturopath in California. Many of my observations and research of lifeblood does not necessary agree with teaching of Dr. Young. I would like to find out if on line course and one year of consultation would give me the same materials that you offer for 80 hours course.At this point I can't travel for two weeks I'm in school. But I don't mind to learn on line.Eventually I would like to meet you in person end continue my education with you.So my question to you is, what is the most comprehensive course that you offer that I could study either on line or with the materials that you can send it to me?

The most comprehensive way is the 80 hours course. If you have already Experience in microscopy I can offer this for you also online. In that Way forget about the hours, I can offer to learn it in the right way, and this is the german way, same as Prof. Enderlein did. By the way I'm German and learned Live Blood Analysis (http://www.dreddyclinic.com/integrated_med/live_blood.php) in Germany. There good books about in German, but almost nothing in English.

We discuss in this course also a lot of nutrition, treatments to change The imbalances.

After I receive your application form and the course fee, we can start online. The course will also include a CD with ppt presentation of the course and many pictures with explanation. 2 Scripts are also included one more focused on the theory, the another one more on the understanding and interpretation of the images what you see in the microscope or on the monitor with your patient. You can use them daily for Your study, but you can send me to another email address also your images (small images!) and we can discuss this together.

Live Blood Analysis (http://www.dreddyclinic.com/integrated_med/live_blood.php) uses a drop of live blood from the patient's finger that has not been killed by staining, and viewed under a special microscope using a darkfield condenser. This enables the blood sample to be illuminated from the sides, making the various components phosphoresce behind a dark background. This makes it possible to see very small particles, smaller than a cell that would not normally be visible under a normal light microscope. All the living components of the blood are seen clearly, and can be viewed by the patient and therapist using a video camera and a dedicated monitor.

The examination of live blood is valuable for the early detection of serious health conditions. It is possible to see at what stage of pathological development the body is in, simply from using one drop of blood.

Because the precursors to serious health imbalances may be observed in the state of ever-present floras found in the blood, health imbalances may be averted by reading these early warning signs and making the necessary changes that will allow one to rebalance the physiology. These markers are also applicable in the course of tracking the progression and reversal of degenerative conditions that may already be in motion.

The observations of these floras are made using what is known as a Darkfield microscope (http://www.dreddyclinic.com/integrated_med/live_blood.php). When utilizing today's conventional approaches to analyze blood, the standard methods are to use either stains, which make certain factors in the blood visible which would not be otherwise visible, or the electron microscope, which provides ultrahigh magnifications. The limitation of both of the preceding approaches is that the blood is effectively killed through the processes utilized in observation. In a Darkfield, the blood is stained with light frequencies, which allow the blood to remain alive and active, giving many otherwise unobtainable clues as to the relative health of the blood, thereby, the whole organism.

We have entered into a new era of scientific discovery. As the horse gave way to the horseless carriage, so must science now accommodate a new understanding of the body as a whole.

Edgar Cayce, the seer of Virginia Beach, predicted in the 1930's that in the future, a person's state of health would be determined by the evaluation of one drop of blood. This time has arrived!

Through the advent of technological advances in microscopy, new discoveries have been proven by such leading researchers as Royal Rife, Gaston Naessans, Dr. Gunther Enderlein, Dr. Majid Ali, M.D. and many others. In the rapidly emerging field of what is known as live cell analysis, an understanding of biology as a holistic science has emerged. Health imbalances in the body may be averted by observing the state of ever-present floras found in the blood and by correcting the milieu that allows the floras to remain in their regulatory forms or to move into pathogenicity. Or conversely, to be reduced from pathogenic forms back down to regulators. These observations are made in what is known as a darkfield.

Under dark-field examination, the various materials making up the structure of the cell or microorganism under view cause it to appear to glow and emit its own light. Since fine structures often cannot be seen when they appear in front of a bright background, illuminating them from the side and viewing them on a black background lights them up and provides contrast and super fine resolution when plan achromat oil immersion iris diaphragm objectives are used. The background is black because the direct or transmitted light from the condenser is passing around the objective and not directly into it (http://www.dreddyclinic.com/integrated_med/live_blood.php).

The only light that is seen is light that is reflected off of the sides and surfaces of the particles. What are seen are illuminated particles on a black background.

This provides a very clear view of the minutest forms, as the eye's potential to differentiate is not overwhelmed by background light and light passing through the sample. Viewing blood in a dark-field is a very useful adjunct when evaluating and addressing the traumatic factors in the total life picture of the individual. The advanced phases of the life-cycle of the colloidal microorganisms are at the very deepest level of causes of blood imbalance and other organism aberrations

For a long time many researchers and doctors believed, and many still do, that blood is sterile. Professor Dr. Gunter Enderlein after numerous years of research, proved otherwise. He showed using darkfield microscopy (http://www.dreddyclinic.com/integrated_med/live_blood.php), that the serum of all people and warm-blooded animals are alive with many moving 'particles'. He called these particles ENDOBIONTS (from the Greek "endon" = internal and "bios" = life).

When you first look at a live blood sample under a microscope or on a monitor you cannot fail to see a multitude of moving, living particles. These are the Endobionts, and are an important part of health.

There are a wide variety of different Endobionts in the blood. In fact, from the simplest apathogenic (non-disease forming) PROTIT, they can change forms into pathological (disease causing) species, depending on how much the pH (acidity-alkalinity) of the blood is changed.

The higher the acidity, the more pathogenicity, and the more likelihood of developing a chronic, degenerative disease process over time. The wonderful world of Live Blood Analysis can enable you to see the different forms in the blood, and to therefore determine how far ahead you are in the disease process.

Prof. Enderlein discovered that these Endobionts change into different forms as the internal milieu changes. The more the metamorphosis (different changes), the greater the probability of disease. The pH of our blood is determined by the food we eat, and the nutrients we take in daily, as well as other factors such as stress and pollutants.

Fast and refined foods and concentrated protein foods all lead to acidic blood which triggers the Endobiont to change to more pathogenic forms.

All microbes partake in a natural developmental cycle, that begins with the PRIMITIVE PHASE which is microscopically invisible; this changes into the BACTERIAL PHASE; and finally culminates in the FUNGAL PHASE, which is the most pathogenic stage. This is the theory of PLEOMORPHISM (many forms), as opposed to monomorphism (one form).

I had a live blood analysis done a year ago through Anthony Robbins "Life Mastery" week long program. I am looking to have this done again and found you on the internet. Is this something you could help me with?